| Literature DB >> 32193289 |
Yi Hu1, Huimin Liu1,2, Chuanfeng Fang1,3, Chen Li1,4, Fjorela Xhyliu5, Hayley Dysert6, Juraj Bodo7, Gabriel Habermehl7, Benjamin E Russell7, Wenjun Li1,2, Marcia Chappell7, Xiaofeng Jiang3, Sarah L Ondrejka7, Eric D Hsi7, Jaroslaw P Maciejewski8, Qing Yi1, Kenneth C Anderson9, Nikhil C Munshi9,10, Geyou Ao5, Jason N Valent6, Jianhong Lin11, Jianjun Zhao12.
Abstract
Multiple myeloma is an incurable refractory hematologic malignancy arising from plasma cells in the bone marrow. Here we investigated miR-26a function in multiple myeloma and tested single-wall carbon nanotube delivery of miR-26a in vitro and in vivo. miR-26a was downregulated in patients with multiple myeloma cells compared with plasma cells from healthy donors. miR-26a overexpression inhibited proliferation and migration and induced apoptosis in multiple myeloma cell lines. To identify the targets of miR-26a, RPMI8226-V-miR-26-GFP and RPMI8226-V-GFP cells were cultured using stable isotope labeling by amino acids in cell culture (SILAC) medium, followed by mass spectrometry analysis. In multiple myeloma cells overexpressing miR-26a, CD38 protein was downregulated and subsequently confirmed to be a direct target of miR-26a. Depletion of CD38 in multiple myeloma cells duplicated the multiple myeloma inhibition observed with exogenous expression of miR-26a, whereas restoration of CD38 overcame the inhibition of miR-26a in multiple myeloma cells. In a human multiple myeloma xenograft mouse model, overexpression of miR-26a inhibited CD38 expression, provoked cell apoptosis, and inhibited cell proliferation. Daratumumab is the first CD38 antibody drug for monotherapy and combination therapy for patients with multiple myeloma, but eventually resistance develops. In multiple myeloma cells, CD38 remained at low level during daratumumab treatment, but a high-quality response is sustained. In daratumumab-resistant multiple myeloma cells, CD38 expression was completely restored but failed to correlate with daratumumab-induced cell death. Therefore, a therapeutic strategy to confer selection pressure to maintain low CD38 expression in multiple myeloma cells may have clinical benefit. SIGNIFICANCE: These results highlight the tumor suppressor function of miR-26a via its targeting of CD38 and suggest the therapeutic potential of miR-26a in patients with multiple myeloma. ©2020 American Association for Cancer Research.Entities:
Year: 2020 PMID: 32193289 PMCID: PMC7231653 DOI: 10.1158/0008-5472.CAN-19-1077
Source DB: PubMed Journal: Cancer Res ISSN: 0008-5472 Impact factor: 12.701